成都工业学院学报
成都工業學院學報
성도공업학원학보
Journal of Chengdu Technological University
2013年
2期
1-5
,共5页
雷凯%刘祥均%陈俐娟%杨明理%向明礼
雷凱%劉祥均%陳俐娟%楊明理%嚮明禮
뢰개%류상균%진리연%양명리%향명례
表皮生长因子受体%不可逆抑制剂%T790M突变%密度泛函理论
錶皮生長因子受體%不可逆抑製劑%T790M突變%密度汎函理論
표피생장인자수체%불가역억제제%T790M돌변%밀도범함이론
EGFR%Irreversible Inhibitor%T790M Mutation%Density Functional Theory
为深究WZ系列抑制剂强效抑制突变型表皮生长因子受体( T790M EGFR)的内在机制,用密度泛函理论( DFT)在B3LYP/6-31G(d)计算水平上对进入临床试验阶段的T790M EGFR不可逆抑制剂HKI-272及WZ系列抑制剂进行了研究。结果表明,WZ系列抑制剂在参与Michael加成反应的能力、与T790M EGFR形成的氢键的强度等方面,都优于HKI-272。抑制剂中的参与形成氢键的氢键供体N原子所带的NBO电荷与抑制剂的抗肿瘤功效高度相关。
為深究WZ繫列抑製劑彊效抑製突變型錶皮生長因子受體( T790M EGFR)的內在機製,用密度汎函理論( DFT)在B3LYP/6-31G(d)計算水平上對進入臨床試驗階段的T790M EGFR不可逆抑製劑HKI-272及WZ繫列抑製劑進行瞭研究。結果錶明,WZ繫列抑製劑在參與Michael加成反應的能力、與T790M EGFR形成的氫鍵的彊度等方麵,都優于HKI-272。抑製劑中的參與形成氫鍵的氫鍵供體N原子所帶的NBO電荷與抑製劑的抗腫瘤功效高度相關。
위심구WZ계렬억제제강효억제돌변형표피생장인자수체( T790M EGFR)적내재궤제,용밀도범함이론( DFT)재B3LYP/6-31G(d)계산수평상대진입림상시험계단적T790M EGFR불가역억제제HKI-272급WZ계렬억제제진행료연구。결과표명,WZ계렬억제제재삼여Michael가성반응적능력、여T790M EGFR형성적경건적강도등방면,도우우HKI-272。억제제중적삼여형성경건적경건공체N원자소대적NBO전하여억제제적항종류공효고도상관。
WZ-series irreversible inhibitors are much more potent against T790M EGFR than HKI-272, one of the inhibitors currently under clinical development. All of them were investigated at the B3LYP/6-31G(d) level by employing G03 so as to reveal the essential factors vital for the potent antitumor activities of the WZ-series inhibitors. It was demonstrated that the WZ-series inhibitors are superior to HKI-272 in the capability to participate in Michael addition reaction. It could be speculated from the calculated results that the strength of H-bond formed between WZ-series inhibitors and T790M EGFR would be stronger than that between HKI-272 and the mutant EGFR. It is worth to note that the values of NBO charge of the H-bond donor in the inhibitors are highly relevant to the antitumor activities of the inhibitors.
